Hostname: page-component-cd9895bd7-hc48f Total loading time: 0 Render date: 2024-12-26T08:33:04.410Z Has data issue: false hasContentIssue false

Symposium on ‘Geographical and geological influences on nutrition’ Iodine deficiency in industrialised countries

Conference on ‘Over- and undernutrition: challenges and approaches’

Published online by Cambridge University Press:  08 December 2009

Michael B. Zimmermann*
Affiliation:
Human Nutrition Laboratory, Swiss Federal Institute of Technology Zürich, Schmelzbergstrasse 7, LFV E19, CH-8092Zürich, Switzerland Division of Human Nutrition, Wageningen University, Wageningen, The Netherlands
*
Corresponding author: Michael B. Zimmermann, fax +41 44 632 1470, email michael.zimmermann@ilw.agrl.ethz.ch
Rights & Permissions [Opens in a new window]

Abstract

Iodine deficiency is not only a problem in developing regions; it also affects many industrialised countries. Globally, two billion individuals have an insufficient iodine intake, and approximately 50% of continental Europe remains mildly iodine deficient. Iodine intakes in other industrialised countries, including the USA and Australia, have fallen in recent years. Iodine deficiency has reappeared in Australia, as a result of declining iodine residues in milk products because of decreased iodophor use by the dairy industry. In the USA, although the general population is iodine sufficient, it is uncertain whether iodine intakes are adequate in pregnancy, which has led to calls for iodine supplementation. The few available data suggest that pregnant women in the Republic of Ireland and the UK are now mildly iodine deficient, possibly as a result of reduced use of iodophors by the dairy industry, as observed in Australia. Representative data on iodine status in children and pregnant women in the UK are urgently needed to inform health policy. In most industrialised countries the best strategy to control iodine deficiency is carefully-monitored salt iodisation. However, because approximately 90% of salt consumption in industrialised countries is from purchased processed foods, the iodisation of household salt only will not supply adequate iodine. Thus, in order to successfully control iodine deficiency in industrialised countries it is critical that the food industry use iodised salt. The current push to reduce salt consumption to prevent chronic diseases and the policy of salt iodisation to eliminate iodine deficiency do not conflict; iodisation methods can fortify salt to provide recommended iodine intakes even if per capita salt intakes are reduced to <5 g/d.

Type
Research Article
Copyright
Copyright © The Author 2009

Abbreviations
NHANES

National Health and Nutrition Examination Survey

TSH

thyroid-stimulating hormone

UI

urinary iodine concentration

Many industrialised countries are areas of historical iodine deficiency and goitre

Iodine (as iodide) is widely but unevenly distributed in the earth's environment. In many regions leaching from glaciation, flooding and erosion have depleted surface soils of iodide and most iodide is found in the oceans. Iodide ions in seawater are oxidised to elemental iodine, which volatilises into the atmosphere and is returned to the soil by rain, completing the cycle(Reference Goldschmidt1). However, iodine cycling in many regions is slow and incomplete, leaving soils and drinking water depleted of iodine. Crops grown in these soils will be low in iodine and human populations and animals consuming food grown in these soils become iodine deficient. Iodine-deficient soils are common in industrialised countries; well-known examples are the Alpine region of Europe, the Midwest in North America, southern Australia and inland areas of western England and Wales. Iodine deficiency and goitre in these areas persists until iodine enters the food chain through the addition of iodine to foods (e.g. iodisation of salt) or dietary diversification introduces foods produced outside the iodine-deficient area.

Iodine is an essential component of the hormones thyroxine and triiodothyronine produced by the thyroid gland(Reference Zimmermann, Jooste and Pandav2). Thyroid hormones, and therefore iodine, are essential for mammalian life. In 1917 it was shown that thyroid enlargement (goitre) is caused by iodine deficiency and can be prevented by iodine supplementation(Reference Marine and Kimball3). Goitre prophylaxis through salt iodisation was first introduced in industrialised countries (Switzerland and the USA) in the early 1920s(Reference Zimmermann4). In 1980 the first global estimate from WHO on the prevalence of goitre was reported; it was estimated that 20–60% of the world's population were iodine deficient and/or goitrous, with most of the burden in developing countries. During the period of 1970–1990 it was shown in controlled studies in iodine-deficient regions that iodine supplementation not only eliminates new cases of cretinism but also reduces infant mortality and improves cognitive function in the rest of the population(Reference Hetzel5). Programmes to correct iodine deficiency were considered to have clear political appeal because its human, economic and social consequences could be averted by a low-cost intervention, universal salt iodisation. Since 1990 elimination of iodine deficiency has been an integral part of national nutrition strategies in most developing countries. In contrast, it has received little attention from public health authorities in many industrialised countries.

Dietary sources, absorption and requirements

The native iodine content of most foods and beverages is low. In general, commonly-consumed foods provide 3–80 μg per serving(Reference Pennington, Schoen and Salmon6, Reference Haldimann, Alt and Blanc7). Foods of marine origin have higher iodine contents because marine plants and animals concentrate iodine from seawater. In the USA the median intake of iodine from food in the mid-1990s was estimated to be 240–300 μg/d for men and 190–210 μg/d for women(8). Major dietary sources of iodine in the USA are bread and milk(Reference Pearce, Pino and He9). In Switzerland, based on direct food analysis, mean intake of dietary iodine is approximately 140 μg/d, mainly from bread and dairy products(Reference Haldimann, Alt and Blanc7). In many countries the use of iodised salt in households for cooking and at the table provides additional iodine. The iodine content of foods is also influenced by iodine-containing compounds used in irrigation, fertilisers and livestock feed. Iodophors used for cleaning milk cans and teats can increase the native iodine content of dairy products. Traditionally, iodate was used in bread making as a dough conditioner, but it is being replaced by non-iodine-containing conditioners, such as bromate. Dietary supplements often contain iodine. Based on data from National Health and Nutrition Examination Survey (NHANES) III (1988–1994) it has been estimated that supplements containing iodine are taken by 12% of men and 15% of non-pregnant women, the median intake of iodine from supplements being approximately 140 μg/d for adults(8). Other sources of iodine include water purification tablets, radiographic contrast media, medicines (e.g. amiodarone) and skin disinfectants (e.g. povidone-iodine contains approximately 10 mg/ml).

Iodine is ingested in several chemical forms. Iodide is rapidly and nearly completely absorbed in the stomach and duodenum. Iodate, widely used in salt iodisation, is reduced in the gut and absorbed as iodide. In healthy adults the absorption of iodide is >90%(Reference Nath, Moinier and Thuillier10). Organically-bound iodine is typically digested and the released iodide absorbed. The body of a healthy adult contains 15–20 mg iodine, of which 70–80% is in the thyroid. In chronic iodine deficiency the iodine content of the thyroid may fall to <20 μg(Reference Zimmermann11). In iodine-sufficient areas the adult thyroid traps approximately 60 μg iodine/d to balance losses and maintain thyroid hormone synthesis(Reference Zimmermann11). Iodine comprises 65 and 59% of thyroxine and triiodothyronine by weight respectively. Degradation of thyroxine and triiodothyronine in the periphery releases iodine that enters the plasma iodine pool and can be taken up by the thyroid or excreted by the kidney(Reference Zimmermann11). Of the ingested iodine >90% is ultimately excreted in the urine. WHO recommendations for iodine intake are shown in Table 1; the WHO recommended nutrient intake for iodine is the intake estimated to cover the needs of ‘nearly all’ healthy individuals at the specified life stage(12).

Table 1. WHO recommendations for iodine intake (μg/d)(12) by age or population group

RNI, recommended nutrient intake.

Methods to assess iodine status

Four methods are generally recommended for assessment of iodine nutrition in populations(12): the goitre rate; urinary iodine concentration (UI); blood thyroid-stimulating hormone (TSH); blood thyroglobulin. These indicators are complementary, in that UI is a sensitive indicator of recent iodine intake (days) and thyroglobulin shows an intermediate response (weeks to months), whereas changes in the goitre rate reflect long-term iodine nutrition (months to years). These methods have recently been extensively reviewed(Reference Zimmermann13). WHO recommends the use of total goitre rate to define severity of iodine deficiency in populations (surveys are usually conducted in school-age children) with the following criteria: <5%, iodine sufficiency; 5·0–19·9%, mild deficiency; 20·0–29·9%, moderate deficiency; >30%, severe deficiency(12). The median UI from a representative sample of spot urine collections from different population groups is the most common way to classify a population's iodine status (Table 2). The median UI is recommended for assessing iodine nutrition in pregnant women, and recently WHO have recommended 150–249 μg/l as the median UI that indicates adequate iodine intake during pregnancy(12) (Table 2). A collection method and a new reference range for UI in newborns in the first week after birth has recently become available(Reference Corey and Zimmermann14). Although UI does not provide direct information on thyroid function, a low value suggests that a population is at higher risk of developing thyroid disorders.

Table 2. WHO epidemiological criteria for the assessment of iodine nutrition in a population based on medians or ranges of urinary iodine concentrations (μg/l)(12)Footnote *

* There is no information about iodine nutrition for pregnant and lactating women in the WHO assessment table, and the upper limits of the median urinary iodine for lactating women and children <2 years of age are not specified.

The values for median urinary iodine are lower than the iodine requirements, because of the iodine excreted in breast milk.

In excess of the amount needed to prevent and control iodine deficiency.

TSH is used in many industrialised countries for routine newborn screening to detect congenital hypothyroidism; such screening offers a sensitive indicator of iodine nutrition in the newborn period(12). Newborn TSH is an important measure because it reflects iodine status during a period when the developing brain is particularly sensitive to iodine deficiency. Serum TSH concentrations are transiently increased in iodine-deficient infants for the first few weeks of life, a condition termed transient newborn hypothyroidism. In areas of iodine deficiency an increase in transient newborn hypothyroidism, indicated by >3% of newborn TSH values above the threshold of 5 mU/l whole blood collected 3–4 d after birth, suggests iodine deficiency in the population(12). Recent data from a large representative Swiss study suggest that newborn TSH is a sensitive indicator of even marginal iodine nutrition in pregnancy(Reference Zimmermann, Aeberli and Torresani15). A new assay for thyroglobulin has been developed for dried blood spots taken by a finger prick(Reference Zimmermann, de Benoist and Corigliano16), simplifying collection and transport. Dried blood spot thyroglobulin has been shown to be a sensitive measure of iodine status(Reference Zimmermann, de Benoist and Corigliano16, Reference Knudsen, Bülow and Jørgensen17) and recently a reference standard and an international reference range in iodine-sufficient schoolchildren (4–40 μg/l) has been made available(Reference Zimmermann, de Benoist and Corigliano16). In contrast, thyroid hormone concentrations are generally poor indicators of iodine status(12), unless iodine deficiency is severe.

Epidemiology of iodine deficiency in industrialised countries

Only a few countries (Switzerland, some of the Scandinavian countries, Australia, the USA and Canada) were recognised as being clearly iodine sufficient before 1990. Since then, globally, the number of households using iodised salt has risen from <20% to >70%, dramatically reducing iodine deficiency(Reference Delange, Bürgi and Chen18). Currently, WHO estimates that approximately two billion individuals have an insufficient iodine intake, including one-third of all school-age children(Reference de Benoist, McLean and Andersson19) (Table 3). The WHO prevalence data emphasise that iodine deficiency is not only a problem of developing countries; the highest prevalence of iodine deficiency is in Europe (52·0%), where the household coverage with iodised salt is the lowest (approximately 25%), and many of these countries have weak or non-existent control programmes for iodine-deficiency disorders(Reference Andersson, de Benoist, Darnton-Hill and Delange20). There are several limitations to these WHO prevalence data. First, extrapolation from a population indicator (median UI) to define the number of individuals affected is problematic, e.g. a country in which children have a median UI of 100 μg/l would be classified as being iodine sufficient, yet at the same time 50% of children would be classified as having inadequate iodine intakes. Second, nationally-representative surveys represent only 60% of the global population included in the WHO data, and sub-national data may under- or overestimate the extent of iodine deficiency(Reference de Benoist, McLean and Andersson19). Finally, there are insufficient data from the majority of the countries to estimate the prevalence of iodine deficiency in pregnant women.

Table 3. Prevalence of iodine deficiency (total number (millions) and percentage) in the general population (all age-groups) and in school-age children (6–12 years) in 2007(Reference de Benoist, McLean and Andersson19)

* 193 WHO member states.

Based on population estimates for 2006(83).

Effects of mild-to-moderate iodine deficiency

Pregnancy

Iodine deficiency, when severe, has multiple adverse effects on growth and development in animals and human subjects, collectively termed the iodine-deficiency disorders(Reference Marine and Kimball3, Reference Zimmermann4). The adverse effects on pregnancy of mild iodine deficiency, typical of industrialised countries, remain unclear. Six controlled trials of iodine treatment in pregnant women with iodine deficiency have been conducted in Europe(Reference Romano, Jannini and Pepe21Reference Antonangeli, Maccherini and Cavaliere26). Overall, these studies suggest that in areas of mild-to-moderate iodine deficiency the maternal thyroid is able to adapt to meet the increased thyroid hormone requirements of pregnancy(Reference Zimmermann27). Although supplementation in these studies was generally found to be effective in minimising an increase in thyroid size during pregnancy, only two of the six studies report that maternal TSH is lower (within the normal reference range) with supplementation, and none of the studies show a marked impact of supplementation on maternal and newborn total or free thyroid hormone concentrations(Reference Zimmermann27). Thyroid hormone concentrations may be the best surrogate biochemical marker for healthy fetal development. Thus, the results of these trials are reassuring. However, because none of the trials measured long-term clinical outcomes such as maternal goitre or infant development, the potential adverse effects of mild-to-moderate iodine deficiency during pregnancy remain uncertain. In industrialised countries with iodine deficiency it has often been suggested that pregnancy is an environmental factor contributing to a higher prevalence of goitre and thyroid disorders in women, compared with men. However, the data to support this premise are scarce. In European studies data from an uncontrolled prospective study in ten women(Reference Glinoer, Lemone and Bourdoux28), a retrospective study(Reference Rotondi, Amato and Biondi29) and a cross-sectional study in smoking women(Reference Knudsen, Bulow and Laurberg30) suggest goitres formed during pregnancy may only partially regress after parturition.

Childhood

There have been many cross-sectional studies comparing cognition and/or motor function in children from chronically iodine-deficient and iodine-sufficient areas, including children from European backgrounds(Reference Vermiglio, Sidoti and Finocchiaro31Reference Vermiglio, Lo Presti and Moleti35). These cross-sectional studies generally report reduced intellectual function and motor skills in children from iodine-deficient areas. However, observational studies are often confounded by other factors that affect child development. Furthermore, these studies could not distinguish between the persistent effects of in utero iodine deficiency and the effects of current iodine status. Two meta-analyses have reported on this issue(Reference Bleichrodt, Born and Stanbury36, Reference Qian, Wang and Watkins37), but they have included mainly data from regions of chronic severe iodine deficiency; in such areas populations experience a mean reduction in intelligence quotient of 12–13·5 points.

In a recent placebo-controlled double-blind 6-month intervention trial 10–12-year-old children with moderate iodine deficiency (n 310) in Albania were randomised to receive either 400 mg iodine as oral iodised oil or placebo. It was found that compared with placebo iodine treatment improves performance on tests of information processing, fine motor skills and visual problem solving(Reference Zimmermann, Connolly and Bozo38). These findings have recently been confirmed in mildly-iodine-deficient New Zealand children(Reference Gordon, Rose and Skeaff39). Thus it appears that in children born and raised in areas of moderate iodine deficiency cognitive impairment is at least partially reversible by iodine repletion(Reference Zimmermann, Connolly and Bozo38, Reference Gordon, Rose and Skeaff39). In addition, recent controlled studies clearly demonstrate that iodine repletion in school-age children with iodine deficiency increases insulin-like growth factor-1 and insulin-like growth factor-binding protein-3 concentrations; in children who have moderate-to-severe deficiency their somatic growth is improved(Reference Zimmermann, Jooste and Mabapa40). Chronic iodine deficiency increases the TSH concentration and produces a thyroid hormone pattern consistent with subclinical hypothyroidism(Reference Zimmermann11), and subclinical hypothyroidism may increase the risk of CVD. Iodised oil rapidly normalises the increased TSH concentrations found in individuals who are iodine-deficient(Reference Zimmermann11) and thus corrects subclinical hypothyroidism. An uncontrolled study has reported that iodine treatment of German adolescents who are goitrous decreases plasma cholesterol concentrations(Reference Rönnefarth, Kauf and Deschner41). A recent controlled study has reported that in children with moderate iodine deficiency and elevated TSH concentrations as a result of iodine deficiency iodine treatment of improves their lipid profile and reduces their insulin (C-peptide) levels compared with controls(Reference Zimmermann, Aeberli and Melse-Boonstra42). This previously unrecognised benefit of iodine prophylaxis may be important because iodine deficiency remains common in many industrialised countries with increasing rates of obesity and CVD.

Treatment and prevention

Salt fortification with iodine

In the majority of industrialised countries affected by iodine deficiency the most effective way to control iodine deficiency is through salt iodisation(12). Salt iodisation is the recommended strategy for control of iodine deficiency because: (1) salt is one of few foodstuffs consumed by virtually every individual; (2) salt intake is fairly consistent through the year; in many countries salt production and importation is limited to a few sources; (3) iodisation technology is simple and relatively inexpensive to implement; (4) the addition of iodine to salt does not affect its colour or taste; (5) the quantity of iodine in salt can be simply monitored at the production, retail and household levels. WHO/UNICEF/International Council for the Control of Iodine Deficiency Disorders recommends that iodine is added at a level of 20–40 mg iodine/kg salt, depending on local salt intake(12). Salt iodisation remains the most cost-effective way of delivering iodine and of improving cognition in populations who are iodine deficient(Reference Engle, Black and Behrman43). Worldwide, the annual costs of salt iodisation are estimated to be US$ 0·02–0·05 per child covered, and the costs per child death averted are US$ 1000 and per disability-adjusted life-year gained are US$ 34–36(Reference Caulfield, Richard, Rivera, Jamison, Breman, Measham, Alleyne, Claeson, Evans, Jha, Mills and Musgrove44).

The importance of food industry use of iodised salt in industrialised countries

WHO recommends universal salt iodisation to control iodine deficiency(12). Universal salt iodisation is a term used to describe the iodisation of all salt for human (food industry and household) and livestock consumption. Although the ideal, even in countries with successful salt iodisation programmes, universal salt iodisation is rarely achieved, as many countries do not iodise all salt for livestock and food industries are often reluctant to use iodised salt. The limited use of iodised salt by the food industry is one of the main reasons for iodine deficiency in many industrialised countries. In countries such as England and Denmark household salt, i.e. salt for cooking and table use, contributes only 8–15% to total salt intakes; most of the remainder comes from purchased processed foods(Reference Sanchez-Castillo, Warrender and Whitehead45, Reference Andersen, Rasmussen and Larsen46). Thus, in industrialised countries, where on average total adult per capita salt consumption is approximately 10 g/d, only about 1 g household salt is consumed daily(Reference Andersen, Rasmussen and Larsen46). If the food industry uses non-iodised salt and only household salt is iodised (at WHO recommended levels of 20 mg iodine/kg salt), then total iodine intake from iodised salt will only be approximately 20 μg/d, far below the daily requirement for all age-groups. Thus, in order to successfully control iodine deficiency in industrialised countries it is critical to convince the food industry to begin to use iodised salt in their products. For example, in The Netherlands all salt used by the baking industry is iodised, and this source is the major contributor to iodine sufficiency in the country(Reference Andersson, de Benoist, Darnton-Hill and Delange20). Switzerland's long-running iodised salt programme has been successful partly because approximately 60% of salt used by the food industry is iodised on a voluntary basis. As iodine at μg/g levels in iodised salt does not cause colour or flavour changes in any foods and in most countries the price difference between iodised and non-iodised salt is negligible, there should be no major barriers to adoption of iodised salt by food manufacturers.

How to reconcile the policy of reducing salt consumption to prevent chronic diseases and the policy of universal salt iodisation to eliminate iodine deficiency

Current WHO recommendations to prevent chronic diseases state that the population average per capita consumption of salt should be <5 g/d (<2 g Na/d)(47). However, the WHO recommendation that salt be fortified with iodine at a level of 20–40 μg/g is based on the assumption of an average salt intake of approximately 10 g/d at the population level(12). Thus, the level of iodine fortification may need to be adjusted by national salt iodisation programmes if health authorities are successful in reducing salt consumption. Since iodisation methods can easily fortify salt with adequate concentrations of iodine to provide recommended iodine intakes even if per capita salt intake falls to <5 g/d, these two important health policies are not in conflict(47). Interaction with food manufacturers in industrialised countries will be fundamental to the success of both salt-reduction strategies and to universal salt iodisation.

Other fortification vehicles

Bread can be an effective vehicle for iodine by including baker's salt enriched with iodine(Reference Seal, Doyle and Burgess48). Although iodising drinking water or irrigation water can also be effective(Reference Squatrito, Vigneri and Runello49), the higher cost and the complexity of monitoring are disadvantages. In Finland iodine-fortified animal fodder has increased the iodine content of foods derived from animal sources. In countries with iodine deficiency iodine should be routinely added to complementary foods or add-on formulas for infants during weaning to provide approximately 90 μg iodine/d(Reference Dunn50).

Iodine supplementation

In some regions iodisation of salt may not be practical for control of iodine deficiency, at least in the short term, and iodine supplements can be used (Table 4)(12). Iodised oil supplements are prepared by esterification of the unsaturated fatty acids in seed or vegetable oils and addition of iodine to the double bonds. It can be given orally or by intramuscular injection(12). The intramuscular route has a longer duration of action, but oral administration is more common because it is simpler. Usual doses are 200–400 mg iodine/year(12) and it is often targeted to women of child-bearing age, pregnant women and children. Its disadvantages are an uneven level of iodine in the body over time and the need for direct contact with individuals with the accompanying increased costs. Iodine can also be given as potassium iodide or potassium iodate as drops or tablets. Single oral doses of potassium iodide monthly (30 mg) or biweekly (8 mg) can provide adequate iodine for school-age children(Reference Todd and Dunn51).

Table 4. Recommendations for iodine supplementation in pregnancy and infancy in areas in which <90% of households are using iodised salt and the median urinary iodine is <100 μg/l in schoolchildren(12)

RNI, reference nutrient intake.

Strategies to prevent or correct deficiency during pregnancy and lactation

For nearly all industrialised countries the primary strategy for sustainable elimination of iodine deficiency in pregnancy remains salt iodisation(12). In countries or regions in which a salt iodisation programme covers ≥90% of households and has been sustained for ≥2 years, and the median UI indicates iodine sufficiency (Table 4), pregnant and lactating women do not need iodine supplementation(12). Several countries with long-standing successful iodised salt programmes have reported an optimal median UI in pregnant women(Reference Zimmermann27). Moreover, in countries affected by mild or moderate iodine deficiency (Republic of Ireland, Germany, Belgium, Italy, Denmark) thyroid volume increases 15–31% during pregnancy, while in iodine-sufficient countries (Finland, The Netherlands) there is little or no increase in thyroid volume during pregnancy(Reference Berghout and Wiersinga52). These data suggest that effective salt iodisation can provide adequate iodine intake during pregnancy, but iodine-containing supplements taken during the prenatal period may have contributed to iodine intakes in these studies.

Implementation of salt iodisation is not always feasible, and non-implementation may result in inadequate iodine supply for women of child-bearing age and pregnant women. In this situation supplementation of these groups should be considered. WHO recommends that countries assess their salt iodisation programmes and then decide whether supplementation is indicated(12). In order to ensure adequate iodine supply during pregnancy women should ideally be provided with adequate iodine intake (≥150 μg/d) for a long period before conception to ensure plentiful intrathyroidal iodine stores(Reference Moleti, Lo Presti and Campolo53). In Italy thyroid function in pregnant women from a mildly-iodine-deficient area who had regularly used iodised salt for ≥2 year before becoming pregnant was compared with that in women who began using iodised salt on becoming pregnant(Reference Moleti, Lo Presti and Campolo53). The findings suggest that prolonged use of iodised salt is associated with better maternal thyroid function, possibly as a result of having greater intrathyroidal iodine stores to draw on during pregnancy. In iodine-deficient countries or regions that have weak iodised salt distribution, i.e. in countries or areas in which <90% of households are using iodised salt and the median UI is <100 μg/l in schoolchildren, supplements should be given to pregnant women, lactating women and infants, according to the strategy shown in Table 4(12).

Iodine nutrition in the industrialised countries: the examples of France, the USA, Australia and the UK and the Republic of Ireland

According to the WHO the highest prevalence of iodine deficiency is in Europe, where the household coverage with iodised salt is the lowest(Reference de Benoist, McLean and Andersson19). It is remarkable that Western Europe has donated substantial funds and effort towards controlling iodine deficiency in less-industrialised countries in Africa and Asia, but has not yet corrected its own problem. Currently, about half the population in Western and Central Europe is mildly iodine deficient(Reference de Benoist, McLean and Andersson19, Reference Andersson, de Benoist, Darnton-Hill and Delange20), and it is likely that unrecognised pockets of more severe deficiency may exist in remote or disadvantaged populations. There are several reasons for this position. Most European nations have weak or non-existent governmental programmes to address iodine deficiency. Awareness of the importance of iodine deficiency is underestimated as many countries have not conducted systematic assessment or monitoring of their populations. Thus, iodine prophylaxis is weaker in most European countries than elsewhere in the world, and laws relating to iodised salt vary widely in Europe, as do the types and amounts of iodine compound used for fortification(Reference Andersson, de Benoist, Darnton-Hill and Delange20).

France

Iodised household salt was introduced in France on a voluntary basis in 1952 (at 10–15 mg sodium iodide/kg salt)(Reference Valeix, Zarebska and Preziosi54). In the mid-1990s iodine status was investigated in a nationally-representative sample of French adults (4860 men aged 45–60 years and 7154 women aged 35–60 years)(Reference Valeix, Zarebska and Preziosi54). The median UI in males and females was reported to be 85 and 82 μg/l respectively, indicating mild iodine deficiency, with an overall goitre rate of 11% for males and 14% for females. The prevalence of individuals with an adequate UI was found to be lowest among 55–60 year olds, with the only 35% of men and 34% of women in this age-group having a UI ≥100 μg/l. The age-related decrease in iodine intake was thought to be a result of a reduction in energy intake with aging and/or increased awareness of the health benefits of reducing Na intake, which may have reduced iodine intake from salt. Median UI were found to display wide marked regional variations; median UI were higher among residents living in the north-west and west than among those living in the centre and east, independent of age and gender. The central region (Auvergne, Limousin) and the north-eastern areas (Alsace, Lorraine, Champagne-Ardennes, Franche-Comté) were found to have the highest percentages (33 and 24 for women and 22 and 23 for men respectively) with UI values <50 μg/l. It was suggested that these regional variations in median UI were a result of variations in the iodine contents of local foodstuffs, as they are dependent on native soil and water iodine content as well as incidental addition of iodine to foods by agricultural practices, including iodine-containing fertilisers, herbicides, disinfectants and/or iodine-supplemented livestock feed(Reference Valeix, Zarebska and Preziosi54).

In contrast to the results in adults, a study of approximately 1500 French children aged 6–14 years conducted in the mid-1990s has reported iodine sufficiency in four areas of France: Lorraine; Rhône-Alpes; Languedoc-Roussillon; Midi-Pyrénées(Reference Caron, Jaffiol and Leclère55). The mean UI was found to be 130 (sd 74) μg/l (only 10% of UI values <50 μg/l), with the prevalence of goitre, determined by ultrasound, being 4·1% in boys and 3·1% in girls.

Two studies in pregnant women in southern France have confirmed iodine deficiency in this group. Mean UI in pregnant women in south-west France (n 347) was found to be 69 (sd 4) μg/l at initial presentation (before 12 weeks of gestation) and 86 (sd 6) μg/l during the ninth month of pregnancy(Reference Caron, Hoff and Bazzi56). During pregnancy a marked decrease was found in free thyroxine and triiodothyronine concentrations, with an increase in TSH and thyroglobulin concentrations. A thyroid ultrasound was performed 1–5 d after delivery in 246 mothers. Thyroid hypertrophy (defined as thyroid volume >18 ml) was found to affect 15·4% of women whose first trimester UI was <50 μg/l, but was present in only 3·5% of women whose first trimester UI was >100 μg/l; 11% of women were found to be goitrous (thyroid volume >22 ml). Similar findings have recently been reported in pregnant women in the third trimester of pregnancy in the Nice area (n 330); median UI was found to be 64 μg/l, with 86% of women having a UI <150 μg/l(Reference Hiéronimus, Bec-Roche and Ferrari57). Median free thyroxine was found to be 12·3 pmol/l, with 41·2% of values being <12 pmol/l. Median TSH was reported to be 1·93 mU/l, with 26·3% having a TSH >2·5 mU/l. Thus, iodine deficiency is common in pregnant women in southern France and may be associated with hypothyroxinaemia and hyperthyrotopinaemia.

The USA

Recent data from the USA indicate the general population is iodine sufficient, and iodine nutrition has improved since the 1960s–1970s when much of the population was consuming excess dietary iodine. Based on the success of the classic iodine supplementation studies in Ohio, general prophylaxis with iodised salt was first introduced in the state of Michigan in 1924(Reference Zimmermann4). In 1948 the USA Endemic Goitre Committee tried to introduce iodised salt to all states by federal law, but the bill failed(Reference Zimmermann4). However, the voluntary use of iodised salt increased across the country and adventitious iodine entered processed foods as iodine-containing compounds were used as bread conditioners and in the dairy industry. These trends were associated with a decline in the prevalence of goitre(Reference Hollowell and Haddow58).

By the 1970s iodine excess had become a greater concern than iodine deficiency, as iodine intakes were estimated to be 150–700 μg/d(Reference Robbins59). In a ten-state study of approximately 36 000 individuals in 1975 the median UI was found to be 250 μg creatinine/g, with the goitre prevalence in all age-groups at 3·1%; a higher prevalence of goitre was found among individuals with high UI values than those with low values(Reference Trowbridge, Hand and Nichaman60). In a subsequent study in approximately 7800 USA children aged 9–16 years the prevalence of goitre was reported to be 6·8%; again with goitre being associated with higher, not lower, UI(Reference Trowbridge, Matovinovic and McLaren61). However, the higher iodine intakes were not found to be associated with discernable thyroid dysfunction.

In the early 1970s the NHANES began to track iodine nutrition in the USA population. NHANES I (1971–1974) reported a median UI of 320 μg/l(Reference Hollowell and Haddow58). Subsequently, results from the USA Total Diet Study suggested a decreased total iodine content of the food supply between 1984 and 1991(Reference Pennington and Schoen62), at least partially because of a reduction in the amount of iodine in milk and the replacement of iodine compounds with bromine salts by the baking industry. Although there are no national data on iodised salt use, it is estimated that only about 60% of salt consumed in the USA is iodised (added as potassium iodide at a concentration of 77 mg iodine/kg salt)(Reference Hollowell and Haddow58).

NHANES III (1988–1994) reported a median UI of 145 μg/l, less than half the median in NHANES I(Reference Hollowell and Haddow58). An increase in individuals with UI concentrations <50 μg/l was found (11·6% in 1988–94 v. 2·4% in 1971–4). However, the frequency of UI concentrations >500 μg/l was reported to be reduced from 27·8% to 5·3%, with the frequency of UI >1000 μg/l falling from 5·3% to 1·3%. Thus, using WHO criteria(12), the data from NHANES III suggested an improvement in iodine status in the USA population, indicated by a sharp decrease in the prevalence of iodine excess, with the median UI in the middle of the range (100–200 μg/l) signifying adequate iodine status. However, concern was expressed that iodine intakes would continue to fall, putting the population at risk of deficiency. This situation has not arisen; in NHANES III the median UI was shown to be stable over the 6 years of sampling and NHANES 2000 and 2001–2002 have reported median UI of 161 μg/l and 168 μg/l respectively(Reference Hollowell and Haddow58). Thus, it appears the iodine intakes in the USA have stabilised. However, in the 2001–2002 NHANES the UI of pregnant women was reported to be 173 (95% CI 75, 229) μg/l, within the range recommended by WHO (150–249 μg/l), but the lower 95% CI was <150 μg/l, partly because of small sample size(Reference Becker and Braverman63). Thus, until additional data become available, in order to ensure adequate iodine intake to maintain euthyroidism for the mother and fetus during pregnancy, the American Thyroid Association has recommended that women receive 150 μg iodine supplements daily during pregnancy and lactation and that all prenatal vitamin–mineral preparations contain 150 μg iodine(Reference Becker and Braverman63).

Australia

Australia is an industrialised country in which mild iodine deficiency has reappeared, after having been controlled for decades mainly by adventitious iodine in milk and milk products. In 1992 the median UI in the Australian population was reported to be >200 μg/l, indicating iodine sufficiency(Reference Li, Eastman and Waite64). A national survey in 2003–4 of schoolchildren in mainland Australia aged 8–10 years (n 1709) has reported a median UI of 104 μg/l(Reference Li, Eastman and Waite64). In New South Wales and Victoria children were found to be mildly iodine deficient, with median UI of 89 μg/l and 73·5 μg/l respectively. Based on WHO reference values by age, 5·6 and 9·3% of boys and girls respectively were found to have increased thyroid volume, but no significant association was demonstrated between UI and thyroid volume. These results indicate marginal iodine intake in the Australian population at the national level, with several of the states being mildly iodine deficient. Tasmania was not included in this survey, but in a study in 2001, before bread fortification with iodine began, the median UI in Tasmanian schoolchildren was reported to be 84 μg/l, with 20% of values <50 μg/l(Reference Guttikonda, Burgess and Hynes65).

These data are supported by a recent cross-sectional study of 815 pregnant women (≥28 weeks of gestation) and 824 newborns in New South Wales(Reference Travers, Guttikonda and Norton66). Spot urine samples were measured for iodine concentration in the women and TSH was measured in newborns at 48–72 h after birth using a sensitive fluoroimmunoassay. The median UI in pregnant women was reported to be 85 μg/l, indicating mild iodine deficiency, with eighteen newborns (2·2%) having TSH values >5 mIU/l. No correlation was found between neonatal TSH and maternal UI, but mothers with a UI <50 μg/l were shown to be 2·6 times (relative risk 2·65 (95% CI 1·49, 4·73)) more likely to have a baby with a TSH level >5 mIU/l.

The major sources of dietary iodine in the Australian diet are thought to be milk and milk products, seafood and iodised salt(Reference Li, Waite and Ma67). However, few individuals purchase iodised salt and, except in Tasmania, few if any food manufacturers use iodised salt in the preparation and manufacture of foods. It has been suggested that for the last 40–50 years the largest source of iodine in the Australian diet has been milk containing iodine residues from sanitising iodophors used in dairying. In a 1975 survey mean iodine concentrations in cow's milk in southern Australia were reported to be 583–593 μg/l(Reference Li, Waite and Ma67). As a result of concerns that high iodine levels in milk could lead to iodine toxicity Food Standards Australia specified a milk iodine limit of 500 μg/l in the Food Standards Code of 1982(68), which led to the replacement of iodophors by chlorine-containing sanitisers. Iodine content of milk samples in Sydney from 2001 to 2004 (thirteen samples per year) were found to be highly variable but generally much lower than in the 1970s, with median concentrations of 140 (range 60–220) μg/l in 2001 and 195 (range 66–412) μg/l in 2004(Reference Li, Waite and Ma67). It was suggested that the reduced amount of iodine in milk is a major reason why iodine deficiency has reappeared in regions of Australia. In 2009 a decision was made by Food Standards Australia New Zealand to address iodine deficiency in the population by requiring the salt in bread to be replaced with iodised salt(69).

The UK and the Republic of Ireland

The re-emergence of iodine deficiency in Australia should raise concern in the UK, as the pattern of a rise and fall in iodine intakes as a result of changes in milk iodine levels may recur in Britain. Studies in the UK in the 1800s reported a high prevalence of goitre and occasional cretinism(Reference Phillips70). By 1900 the English goitre belt was well-defined; it extended from the West Country through Somerset and northwards into Derbyshire and the Peak District, with offshoots into North and South Wales. The high regional goitre rates in adults and children in the 1940s led to recommendations by the Medical Research Council in 1944 and 1948 for a programme of iodised salt throughout the UK, but no action was taken(71). In Oxfordshire the goitre prevalence between 1948 and 1958 was found to be essentially unchanged in boys but increased in girls, from 27% to 40%(Reference Hughes, Rodgers and Wilson72). Goitre remained a health problem into the early 1960s in Sheffield and Wales(Reference Trotter, Cochrane and Benjamin73, Reference Kilpatrick, Milne and Rushbrooke74), as well as in Glasgow, where patients presenting with non-toxic goitre were reported to have low dietary iodine intake and low plasma inorganic iodine concentrations(Reference Phillips70). Although monitoring data are scarce, it appears that since the 1960s the prevalence of iodine deficiency and goitre has fallen in the UK. A 1990 survey has reported the absence of thyroid enlargement in children in a traditionally iodine-deficient area of South Wales(Reference Lazarus, Phillips, Parkes, Delange, Dunn and Glinoer75).

The improvement in iodine intakes dating from the 1960s in the UK may have been a result, at least in part, of increasing iodine intake from milk and milk products. Iodine supplementation of livestock improves their reproductive performance and many UK dairy herds, beginning as early as the 1920s and 1930s, have been given iodine via iodised salt licks and/or iodine-enriched cattle feed(Reference Phillips70). This practice increases the iodine content of milk, particularly during the winter months, when cattle are more dependent on iodine-rich artificial feed. In addition, the use of iodophor disinfectants for cleaning teats and milk tankers and giving iodinated casein to cows to promote lactation have also contributed to higher iodine levels in milk(Reference Phillips70). The simultaneous increase in per capita milk consumption has resulted in the amount of iodine provided by milk in the UK sharply increasing; it was estimated that average daily iodine intake from milk increased between 1930 and 1980 from approximately 5 μg to 25 μg (in summer) and >100 μg (in winter)(Reference Phillips70). The increasing contribution of milk iodine is likely to be a major reason why estimated dietary iodine intakes in the UK increased between 1952 and 1982 from 80 μg to 255 μg/d(Reference Wenlock, Buss and Moxon76).

However, several UK authors have suggested that the increasing trend to replace iodine compounds used in the dairy and baking industries with non-iodine alternatives may be decreasing iodine intakes, similar to the situation that has occurred in Australia(Reference Lazarus and Smyth77Reference Smyth, Hetherton and Smith82). If adventitious dietary iodine falls, the population may be vulnerable to iodine deficiency because iodised salt makes up <5% of all salt consumed in the UK and the Republic of Ireland(Reference Lazarus and Smyth77). Recent measurement of the iodine content in retail salt (thirty-six samples) in Cardiff (Wales) has shown iodine concentrations to be undetectable in thirty-two samples, with two samples, labelled as iodised, containing approximately 20 mg iodine/kg(Reference Lazarus and Smyth77).

Limited data from Scotland(Reference Barnett, Visser and Williams78) and north-east England(Reference Kibirige, Hutchison and Owen79) suggest many pregnant women are iodine deficient. In a study in Middlesbrough (north-east England) in 2000–2001 pregnant women attending the antenatal clinic at 15 weeks of gestation (n 227) and non-pregnant age-matched controls (n 227) were enrolled(Reference Kibirige, Hutchison and Owen79). Sixteen of the pregnant women (7%) and twenty of the non-pregnant controls (8·8%) were found to have UI <50 μg/l, with ninety (40%) of the pregnant women having UI between 50 μg/l and 100 μg/l. The 227 pregnancies resulted in 218 live births and no newborn was reported to have a clearly elevated blood TSH. Although it was suggested that the data indicate borderline iodine deficiency in pregnancy, using the current WHO cut-off value for inadequate iodine intake for this group (150 μg/l)(12) most of the women were clearly iodine deficient.

In the Republic of Ireland the distribution of newborn TSH as a measure of iodine nutrition has been examined in the population(Reference Burns, Mayne and O'Herlihy80). Samples drawn from the National Neonatal Screening Programme were assessed during the years 1995–2006. In 1995–6 the frequency of TSH values >5·0 mIU/l was found to be >3%, suggesting iodine deficiency in the population. However, a marked decline in the proportion of elevated values was observed in the subsequent years. At the same time, a small but significant increase (P<0·001) in mean blood TSH within the 0–5·0 mIU/l interval was observed between 1999 and 2006. It was suggested that the trend towards increasing TSH is of concern and should be monitored carefully. UI was measured in Irish women (n 54) during the first trimester of pregnancy (median 8 weeks of gestation) attending the National Maternity Hospital in Dublin(Reference Nawoor, Burns and Smith81). The samples were taken at different times during the year with thirty-six samples taken in the summer months. The UI were found to show seasonal variation; the median UI in the women being 45 μg/l in summer and 68 μg/l in winter. These values are lower than those in a study of pregnant women in Dublin in the mid-1990s from the same research group(Reference Smyth, Hetherton and Smith82), in which the median UI was reported to be 83 μg/l in summer and 135 μg/l in winter. Although these studies were small, they suggest dietary iodine intake in Irish pregnant women continues to fall well short of WHO recommendations. This outcome is not surprising, as only about 3–4% of total salt sales in Ireland are iodised(Reference Nawoor, Burns and Smith81). Thus, dietary iodine intake in the Irish population depends on consumption of sea fish and marine products, which varies widely among regions and individuals, and milk and dairy products, the iodine content of which varies seasonally and may be decreasing as a result of reduced use of iodophor disinfectants by dairies. As in the UK, relying on unpredictable amounts of iodine in the food supply, driven mainly by commercial rather than health interests, is precarious. The few available data suggest that the Republic of Ireland and the UK are mildly iodine deficient. Representative data on current iodine status in children and pregnant women are urgently needed to inform health policy.

Conclusion

Mild iodine deficiency affects many industrialised countries, including Australia, New Zealand and approximately 50% of continental Europe. It is likely that pregnant women in the Republic of Ireland and the UK are also mildly iodine deficient, but there are few representative data. In most industrialised countries the best strategy to control iodine deficiency is carefully-monitored salt iodisation. However, because approximately 90% of the salt consumption in industrialised countries is from purchased processed foods, it is critical that the food industry use iodised salt. The current push to reduce salt consumption to prevent chronic diseases is not at odds with salt iodisation to eliminate iodine deficiency; as salt intakes fall, the iodine content of salt can be increased to deliver adequate iodine, even if per capita salt intakes are reduced to <5 g/d.

Acknowledgements

The author declares no conflict of interest. The Swiss Federal Institute of Technology in Zürich provided financial support during the researching and writing of this manuscript.

References

1.Goldschmidt, VW (1954) Geochemistry. Oxford: Oxford University Press.Google Scholar
2.Zimmermann, MB, Jooste, PL & Pandav, CS (2008) The iodine deficiency disorders. Lancet 372, 12511262.CrossRefGoogle ScholarPubMed
3.Marine, D & Kimball, OP (1917) The prevention of simple goiter in man. J Lab Clin Med 3, 4048.Google Scholar
4.Zimmermann, MB (2008) Research on iodine deficiency and goiter in the 19th and early 20th centuries. J Nutr 138, 20602063.CrossRefGoogle ScholarPubMed
5.Hetzel, BS (1983) Iodine deficiency disorders (IDD) and their eradication. Lancet ii, 11261129.CrossRefGoogle Scholar
6.Pennington, JAT, Schoen, SA, Salmon, GD et al. (1995) Composition of core foods in the U.S. food supply, 1982–1991. J Food Compost Anal 8, 171217.CrossRefGoogle Scholar
7.Haldimann, M, Alt, A, Blanc, A et al. (2005) Iodine content of food groups. J Food Compost Anal 18, 461471.CrossRefGoogle Scholar
8.Institute of Medicine, Academy of Sciences (2001) Dietary Reference Intakes for Vitamin A, Vitamin K, Arsenic, Boron, Chromium, Copper, Iodine, Iron, Manganese, Molybdenum, Nickel, Silicon, Vanadium, and Zinc. Washington, DC: National Academy Press.Google Scholar
9.Pearce, EN, Pino, S, He, X et al. (2004) Sources of dietary iodine: bread, cows' milk, and infant formula in the Boston area. J Clin Endocrinol Metab 89, 34213424.CrossRefGoogle ScholarPubMed
10.Nath, SK, Moinier, B, Thuillier, F et al. (1992) Urinary excretion of iodide and fluoride from supplemented food grade salt. Int J Vitam Nutr Res 62, 6672.Google ScholarPubMed
11.Zimmermann, MB (2009) Iodine deficiency. Endocr Rev 30, 376408.CrossRefGoogle ScholarPubMed
12.World Health Organization/United Nations Children's Fund/International Council for the Control of Iodine Deficiency Disorders (2007) Assessment of Iodine Deficiency Disorders and Monitoring their Elimination, 3rd ed. Geneva: WHO.Google Scholar
13.Zimmermann, MB (2008) Methods to assess iron and iodine status. Br J Nutr 99, Suppl. 3, S2S9.CrossRefGoogle ScholarPubMed
14.Corey, CM & Zimmermann, MB (2008) Reference values for spot urinary iodine concentrations in iodine-sufficient newborns using a new pad collection method. Thyroid 18, 347352.Google Scholar
15.Zimmermann, MB, Aeberli, I, Torresani, T et al. (2005) Increasing the iodine concentration in the Swiss iodized salt programme markedly improved iodine status in pregnant women and children: a 5-y prospective national study. Am J Clin Nutr 82, 388392.CrossRefGoogle ScholarPubMed
16.Zimmermann, MB, de Benoist, B, Corigliano, S et al. (2006) Assessment of iodine status using dried blood spot thyroglobulin: Development of reference material and establishment of an international reference range in iodine-sufficient children. J Clin Endocrinol Metab 91, 48814887.CrossRefGoogle ScholarPubMed
17.Knudsen, N, Bülow, I, Jørgensen, T et al. (2001) Serum Tg – a sensitive marker of thyroid abnormalities and iodine deficiency in epidemiological studies. J Clin Endocrinol Metab 86, 35993603.Google ScholarPubMed
18.Delange, F, Bürgi, H, Chen, ZP et al. (2002) World status of monitoring iodine deficiency disorders control programmes. Thyroid 12, 915924.CrossRefGoogle Scholar
19.de Benoist, B, McLean, E & Andersson, M (2008) Iodine deficiency in 2007: Global progress since 2003. Food Nutr Bull 29, 195202.CrossRefGoogle ScholarPubMed
20.World Health Organization (2007) Iodine deficiency in Europe [Andersson, M, de Benoist, B, Darnton-Hill, I and Delange, F, editors]. Geneva: WHO.Google Scholar
21.Romano, R, Jannini, EA, Pepe, M et al. (1991) The effects of iodoprophylaxis on thyroid size during pregnancy. Am J Obst Gynecol 164, 482485.CrossRefGoogle ScholarPubMed
22.Pedersen, KM, Laurberg, P, Iversen, E et al. (1993) Amelioration of some pregnancy-associated variations in thyroid function by iodine supplementation. J Clin Endocrinol Metab 77, 10781083.Google ScholarPubMed
23.Glinoer, D, De Nayer, P, Delange, F et al. (1995) A randomized trial for the treatment of mild iodine deficiency during pregnancy: maternal and neonatal effects. J Clin Endocrinol Metab 80, 258269.Google ScholarPubMed
24.Liesenkötter, KP, Göpel, W, Bogner, U et al. (1996) Earliest prevention of endemic goiter by iodine supplementation during pregnancy. Eur J Endocrinol 134, 443448.CrossRefGoogle ScholarPubMed
25.Nohr, SB, Jorgensen, A, Pedersen, KM et al. (2000) Postpartum thyroid dysfunction in pregnant thyroid peroxidase antibody-positive women living in an area with mild to moderate iodine deficiency: is iodine supplementation safe? J Clin Endocrinol Metab 85, 31913198.CrossRefGoogle Scholar
26.Antonangeli, L, Maccherini, D, Cavaliere, R et al. (2002) Comparison of two different doses of iodide in the prevention of gestational goiter in marginal iodine deficiency: a longitudinal study. Eur J Endocrinol 147, 2934.CrossRefGoogle ScholarPubMed
27.Zimmermann, MB (2009) Iodine deficiency in pregnancy and the effects of maternal iodine supplementation on the offspring: a review. Am J Clin Nutr 89, 668S672S.CrossRefGoogle ScholarPubMed
28.Glinoer, D, Lemone, M, Bourdoux, P et al. (1992) Partial reversibility during late postpartum of thyroid abnormalities associated with pregnancy. J Clin Endocrinol Metab 74, 453457.Google ScholarPubMed
29.Rotondi, M, Amato, G, Biondi, B et al. (2000) Parity as a thyroid size-determining factor in areas with moderate iodine deficiency. J Clin Endocrinol Metab 85, 45344537.CrossRefGoogle ScholarPubMed
30.Knudsen, N, Bulow, I, Laurberg, P et al. (2002) Parity is associated with increased thyroid volume solely among smokers in an area with moderate to mild iodine deficiency. Eur J Endocrinol 146, 3943.CrossRefGoogle Scholar
31.Vermiglio, F, Sidoti, M, Finocchiaro, MD et al. (1990) Defective neuromotor and cognitive ability in iodine-deficient schoolchildren of an endemic goiter region in Sicily. J Clin Endocrinol Metab 70, 379384.CrossRefGoogle ScholarPubMed
32.Fenzi, GF, Giusti, LF, Aghini-Lombardi, F et al. (1990) Neuropsychological assessment in schoolchildren from an area of moderate iodine deficiency. J Endocrinol Invest 13, 427431.CrossRefGoogle ScholarPubMed
33.Vitti, P, Aghini Lombardi, F, Antonangeli, L et al. (1992) Mild iodine deficiency in fetal/neonatal life and neuropsychological performances. Acta Med Austriaca 19, Suppl. 1, 5759.Google ScholarPubMed
34.Aghini Lombardi, FA, Pinchera, A, Antonangeli, L et al. (1995) Mild iodine deficiency during fetal/neonatal life and neuropsychological impairment in Tuscany. J Endocrinol Invest 18, 5762.CrossRefGoogle ScholarPubMed
35.Vermiglio, F, Lo Presti, VP, Moleti, M et al. (2004) Attention deficit and hyperactivity disorders in the offspring of mothers exposed to mild-moderate iodine deficiency: a possible novel iodine deficiency disorder in developed countries. J Clin Endocrinol Metab 89, 60546060.CrossRefGoogle ScholarPubMed
36.Bleichrodt, N & Born, MP (1994) A metaanalysis of research on iodine and its relationship to cognitive development. In The Damaged Brain of Iodine Deficiency, pp. 195200 [Stanbury, JB, editor]. New York: Cognizant Communications Corp.Google Scholar
37.Qian, M, Wang, D, Watkins, WE et al. (2005) The effects of iodine on intelligence in children: a meta-analysis of studies conducted in China. Asia Pac J Clin Nutr 14, 3242.Google ScholarPubMed
38.Zimmermann, MB, Connolly, K, Bozo, M et al. (2006) Iodine supplementation improves cognition in iodine-deficient schoolchildren in Albania: a randomized, controlled, double-blind study. Am J Clin Nutr 83, 108114.CrossRefGoogle ScholarPubMed
39.Gordon, RC, Rose, MC, Skeaff, SA et al. (2009) Iodine supplementation improves cognition in mildly iodine-deficient children. Am J Clin Nutr 90, 12641271.CrossRefGoogle ScholarPubMed
40.Zimmermann, MB, Jooste, PL, Mabapa, NS et al. (2007) Treatment of iodine deficiency in school-age children increases IGF-1 and IGFBP-3 concentrations and improves somatic growth. J Clin Endocrinol Metab 92, 437442.CrossRefGoogle ScholarPubMed
41.Rönnefarth, G, Kauf, E, Deschner, F et al. (1996) Therapy of iodine deficiency goiter in adolescents with iodine or a combination of iodine and levothyroxine with special reference to lipid parameters. Klin Padiatr 208, 123128.CrossRefGoogle ScholarPubMed
42.Zimmermann, MB, Aeberli, I, Melse-Boonstra, A et al. (2009) Iodine treatment in children with subclinical hypothyroidism due to chronic iodine deficiency decreases TSH and C-peptide concentrations and improves the lipid profile. Thyroid 19, 10991104.CrossRefGoogle ScholarPubMed
43.Engle, PL, Black, MM, Behrman, JR et al. (2007) Strategies to avoid the loss of developmental potential in more than 200 million children in the developing world. Lancet 369, 229242.CrossRefGoogle ScholarPubMed
44.Caulfield, LE, Richard, SA, Rivera, JA et al. (2006) Stunting, wasting, and micronutrient deficiency disorders. In Disease Control Priorities in Developing Countries, 2nd ed., pp. 551568 [Jamison, DT, Breman, JG, Measham, AR, Alleyne, G, Claeson, M, Evans, DB, Jha, P, Mills, A and Musgrove, P, editors]. New York: Oxford University Press.Google Scholar
45.Sanchez-Castillo, CP, Warrender, S, Whitehead, TP et al. (1987) An assessment of the sources of dietary salt in a British population. Clin Sci (Lond) 72, 95–102.CrossRefGoogle Scholar
46.Andersen, L, Rasmussen, LB, Larsen, EH et al. (2009) Intake of household salt in a Danish population. Eur J Clin Nutr 63, 598604.CrossRefGoogle Scholar
47.World Health Organization (2008) WHO Expert Consultation on Salt as a Vehicle for Fortification. Geneva: WHO.Google Scholar
48.Seal, JA, Doyle, Z, Burgess, JR et al. (2007) Iodine status of Tasmanians following voluntary fortification of bread with iodine. Med J Aust 186, 6971.CrossRefGoogle ScholarPubMed
49.Squatrito, S, Vigneri, R, Runello, F et al. (1986) Prevention and treatment of endemic iodine-deficiency goiter by iodination of a municipal water supply. J Clin Endocrinol Metab 63, 368375.CrossRefGoogle ScholarPubMed
50.Dunn, JT (2003) Iodine should be routinely added to complementary foods. J Nutr 133, 3008S3010S.CrossRefGoogle ScholarPubMed
51.Todd, CH & Dunn, JT (1998) Intermittent oral administration of potassium iodide solution for the correction of iodine deficiency. Am J Clin Nutr 67, 12791283.CrossRefGoogle ScholarPubMed
52.Berghout, A & Wiersinga, W (1998) Thyroid size and thyroid function during pregnancy: an analysis. Eur J Endocrinol 138, 536542.CrossRefGoogle ScholarPubMed
53.Moleti, M, Lo Presti, VP, Campolo, MC et al. (2008) Iodine prophylaxis using iodized salt and risk of maternal thyroid failure in conditions of mild iodine deficiency. J Clin Endocrinol Metab 93, 26162621.CrossRefGoogle ScholarPubMed
54.Valeix, P, Zarebska, M, Preziosi, P et al. (1999) Iodine deficiency in France. Lancet 353, 17661767.CrossRefGoogle ScholarPubMed
55.Caron, P, Jaffiol, C, Leclère, J et al. (1996) Iodine consumption in France. National results of the Thyromobile project in a population of schoolchildren aged 6–14 years. Ann Endocrinol (Paris) 57, 228233.Google Scholar
56.Caron, P, Hoff, M, Bazzi, S et al. (1997) Urinary iodine excretion during normal pregnancy in healthy women living in the southwest of France: correlation with maternal thyroid parameters. Thyroid 7, 749754.CrossRefGoogle ScholarPubMed
57.Hiéronimus, S, Bec-Roche, M, Ferrari, P et al. (2009) Iodine status and thyroid function of 330 pregnant women from Nice area assessed during the second part of pregnancy. Ann Endocrinol (Paris) 70, 218224.CrossRefGoogle ScholarPubMed
58.Hollowell, JG & Haddow, JE (2007) The prevalence of iodine deficiency in women of reproductive age in the United States of America. Public Health Nutr 10, 15321539.CrossRefGoogle ScholarPubMed
59.Robbins, J (1980) Iodine deficiency, excess, and the use of iodine for protection against radioactive iodine. Thyroid Stud 3, 1.Google Scholar
60.Trowbridge, FL, Hand, KA & Nichaman, MZ (1975) Findings relating to goiter and iodine in the Ten-State Nutrition Survey. Am J Clin Nutr 28, 712716.CrossRefGoogle ScholarPubMed
61.Trowbridge, FL, Matovinovic, J, McLaren, GD et al. (1975) Iodine and goiter in children. Pediatrics 56, 8290.CrossRefGoogle ScholarPubMed
62.Pennington, JAT & Schoen, SA (1996) Total Diet Study: estimated dietary intakes of nutritional elements, 1982–1991. Int J Vit Nutr Res 66, 350362.Google ScholarPubMed
63.Public Health Committee of the American Thyroid Association, Becker, DV, Braverman, LE et al. (2006) Iodine supplementation for pregnancy and lactation – United States and Canada: recommendations of the American Thyroid Association. Thyroid 16, 949951.CrossRefGoogle ScholarPubMed
64.Li, M, Eastman, CJ, Waite, KV et al. (2006) Are Australian children iodine deficient? Results of the Australian National Iodine Nutrition Study. Med J Aust 184, 165169.CrossRefGoogle ScholarPubMed
65.Guttikonda, K, Burgess, JR, Hynes, K et al. (2007) Recurrent iodine deficiency in Tasmania, Australia: a salutary lesson in sustainable iodine prophylaxis and its monitoring. J Clin Endocrinol Metab 87, 28092815.CrossRefGoogle Scholar
66.Travers, CA, Guttikonda, K, Norton, CA et al. (2006) Iodine status in pregnant women and their newborns: are our babies at risk of iodine deficiency? Med J Aust 184, 617620.CrossRefGoogle ScholarPubMed
67.Li, M, Waite, KV, Ma, G et al. (2006) Declining iodine content of milk and re-emergence of iodine deficiency in Australia. Med J Aust 184, 307.CrossRefGoogle ScholarPubMed
68.Food Standards Australia (1982) Food Standards Code 1982. Canberra: Australian Government Publishing Service.Google Scholar
69.Food Standards Australia New Zealand (2009) Standard 2.1.1 – Cereals and cereal products. http://www.foodstandards.gov.au/_srcfiles/Standard_2_1_1_Cereals_v112.pdfGoogle Scholar
70.Phillips, DIW (1997) Iodine, milk, and the elimination of endemic goitre in Britain: the story of an accidental public health triumph. J Epidemiol Community Health 51, 391393.CrossRefGoogle ScholarPubMed
71.Medical Research Council Goitre Subcommittee (1944) Endemic goitre in England. Argument for preventive action. Lancet i, 107109.Google Scholar
72.Hughes, DE, Rodgers, K & Wilson, DC (1959) Thyroid enlargement in schoolchildren of North Oxfordshire. Br Med J 1, 280281.CrossRefGoogle ScholarPubMed
73.Trotter, WR, Cochrane, AL, Benjamin, IT et al. (1962) A goitre survey in the Vale of Glamorgan. Br Prev Soc Med 16, 1621.Google Scholar
74.Kilpatrick, R, Milne, JS, Rushbrooke, M et al. (1963) A survey of thyroid enlargement in two general practices in Great Britain. Br Med J 1, 2934.CrossRefGoogle ScholarPubMed
75.Lazarus, JH, Phillips, DIW, Parkes, AB et al. (1993) Status of iodine nutrition in the United Kingdom. In Iodine Deficiency in Europe: A Continuing Concern, pp. 323327 [Delange, F, Dunn, JT and Glinoer, D, editors]. New York: Plenum Press.CrossRefGoogle Scholar
76.Wenlock, RW, Buss, DH, Moxon, RE et al. (1982) Trace nutrients 4. Iodine in British food. Br J Nutr 47, 381390.CrossRefGoogle ScholarPubMed
77.Lazarus, JH & Smyth, PPA (2008) Iodine deficiency in the UK and Ireland. Lancet 372, 888.CrossRefGoogle ScholarPubMed
78.Barnett, CA, Visser, TJ, Williams, F et al. (2002) Inadequate iodine intake of 40% of pregnant women from a region in Scotland. J Endocrinol Invest 25, Suppl., 90.Google Scholar
79.Kibirige, MS, Hutchison, S, Owen, CJ et al. (2004) Prevalence of maternal dietary iodine insufficiency in the north east of England: implications for the fetus. Arch Dis Child Fetal Neonatal Ed 89, 436439.CrossRefGoogle Scholar
80.Burns, R, Mayne, PD, O'Herlihy, C et al. (2008) Can neonatal TSH screening reflect trends in population iodine intake? Thyroid 18, 883888.CrossRefGoogle ScholarPubMed
81.Nawoor, Z, Burns, R, Smith, DF et al. (2006) Iodine intake in pregnancy in Ireland – a cause for concern? Ir J Med Sci 175, 2124.CrossRefGoogle Scholar
82.Smyth, PPA, Hetherton, AMT, Smith, DF et al. (1997) Maternal iodine status and thyroid volume during pregnancy: Correlation with neonatal iodine intake. J Clin Endocrinol Metab 82, 28402843.CrossRefGoogle ScholarPubMed
83.United Nations (2005) World Population Prospects: The 2004 Revision. New York: United Nations; available at http://www.un.org/esa/population/publications/WPP2004/2004Highlights_finalrevised.pdfGoogle Scholar
Figure 0

Table 1. WHO recommendations for iodine intake (μg/d)(12) by age or population group

Figure 1

Table 2. WHO epidemiological criteria for the assessment of iodine nutrition in a population based on medians or ranges of urinary iodine concentrations (μg/l)(12)*

Figure 2

Table 3. Prevalence of iodine deficiency (total number (millions) and percentage) in the general population (all age-groups) and in school-age children (6–12 years) in 2007(19)

Figure 3

Table 4. Recommendations for iodine supplementation in pregnancy and infancy in areas in which <90% of households are using iodised salt and the median urinary iodine is <100 μg/l in schoolchildren(12)